Your search keyword '"Gabriel Melo de Oliveira"' showing total 4 results

1. Combined treatment of heterocyclic analogues and benznidazole upon Trypanosoma cruzi in vivo.

Author

Denise da Gama Jaén Batista, Marcos Meuser Batista, Gabriel Melo de Oliveira, Constança Carvalho Britto, Ana Carolina Mondaine Rodrigues, Chad E Stephens, David W Boykin, and Maria de Nazaré Correia Soeiro

Subjects

Medicine, Science

Abstract

Chagas disease caused by Trypanosoma cruzi is an important cause of mortality and morbidity in Latin America but no vaccines or safe chemotherapeutic agents are available. Combined therapy is envisioned as an ideal approach since it may enhance efficacy by acting upon different cellular targets, may reduce toxicity and minimize the risk of drug resistance. Therefore, we investigated the activity of benznidazole (Bz) in combination with the diamidine prodrug DB289 and in combination with the arylimidamide DB766 upon T. cruzi infection in vivo. The oral treatment of T.cruzi-infected mice with DB289 and Benznidazole (Bz) alone reduced the number of circulating parasites compared with untreated mice by about 70% and 90%, respectively. However, the combination of these two compounds decreased the parasitemia by 99% and protected against animal mortality by 100%, but without providing a parasitological cure. When Bz (p.o) was combined with DB766 (via i.p. route), at least a 99.5% decrease in parasitemia levels was observed. DB766+Bz also provided 100% protection against mice mortality while Bz alone provided about 87% protection. This combined therapy also reduced the tissular lesions induced by T. cruzi infection: Bz alone reduced GPT and CK plasma levels by about 12% and 78% compared to untreated mice group, the combination of Bz with DB766 resulted in a reduction of GPT and CK plasma levels of 56% and 91%. Cure assessment through hemocultive and PCR approaches showed that Bz did not provide a parasitological cure, however, DB766 alone or associated with Bz cured ≥13% of surviving animals.

Published

2011

2. In vitro and in vivo investigation of the efficacy of arylimidamide DB1831 and its mesylated salt form--DB1965--against Trypanosoma cruzi infection

Author

Cristiane França da Silva, Julianna Siciliano de Araújo, Gabriel Melo de Oliveira, Maria de Nazaré Correia Soeiro, Elen Mello de Souza, Abdelbasset A. Farahat, Denise da Gama Jaen Batista, Arvind Kumar, Erica Ripoll Hammer, David W. Boykin, Constança Britto, Zong-ying Liu, Ana Carolina Mondaine Rodrigues, Anissa Daliry, and Patrícia Bernardino da Silva

Subjects

Male, Amidines, Drug Evaluation, Preclinical, lcsh:Medicine, Protozoology, Pharmacology, Biochemistry, Mice, chemistry.chemical_compound, lcsh:Science, Cells, Cultured, Mesylates, Multidisciplinary, biology, Chemistry, Treatment Outcome, Infectious Diseases, Benznidazole, Medicine, Female, Research Article, Biotechnology, Neglected Tropical Diseases, medicine.drug, Chagas disease, Drugs and Devices, Drug Research and Development, Trypanosoma cruzi, Antiprotozoal Agents, Models, Biological, Microbiology, In vivo, parasitic diseases, Parasitic Diseases, medicine, Animals, Chagas Disease, Nifurtimox, Biology, No-Observed-Adverse-Effect Level, Mesylate, Intracellular parasite, lcsh:R, biology.organism_classification, medicine.disease, Amides, In vitro, Pyrimidines, chemistry, Parastic Protozoans, lcsh:Q, Medicinal Chemistry

Abstract

Chagas disease is caused by infection with the intracellular protozoan parasite Trypanosoma cruzi. At present, nifurtimox and benznidazole, both compounds developed empirically over four decades ago, represent the chemotherapeutic arsenal for treating this highly neglected disease. However, both drugs present variable efficacy depending on the geographical area and the occurrence of natural resistance, and are poorly effective against the later chronic stage. As a part of a search for new therapeutic opportunities to treat chagasic patients, pre-clinical studies were performed to characterize the activity of a novel arylimidamide (AIA--DB1831 (hydrochloride salt) and DB1965 (mesylate salt)) against T. cruzi. These AIAs displayed a high trypanocidal effect in vitro against both relevant forms in mammalian hosts, exhibiting a high selectivity index and a very high efficacy (IC(50) value/48 h of 5-40 nM) against intracellular parasites. DB1965 shows high activity in vivo in acute experimental models (mouse) of T. cruzi, showing a similar effect to benznidazole (Bz) when compared under a scheme of 10 daily consecutive doses with 12.5 mg/kg. Although no parasitological cure was observed after treating with 20 daily consecutive doses, a combined dosage of DB1965 (5 mg/kg) with Bz (50 mg/kg) resulted in parasitaemia clearance and 100% animal survival. In summary, our present data confirmed that aryimidamides represent promising new chemical entities against T. cruzi in therapeutic schemes using the AIA alone or in combination with other drugs, like benznidazole.

Published

2012

3. Oral Administration of GW788388, an Inhibitor of Transforming Growth Factor Beta Signaling, Prevents Heart Fibrosis in Chagas Disease

Author

Mariana Caldas Waghabi, Fabiane L. de Oliveira, Gabriel Melo de Oliveira, Tania C. Araújo-Jorge, Sabine Bailly, Jean-Jacques Feige, Wim Degrave, and Elen Mello de Souza

Subjects

Chagas Cardiomyopathy, Male, Chagas disease, Drugs and Devices, lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, Trypanosoma cruzi, Administration, Oral, Inflammation, Cardiovascular, Mice, Transforming Growth Factor beta, In vivo, Fibrosis, Oral administration, parasitic diseases, medicine, Animals, Receptor, biology, lcsh:Public aspects of medicine, Myocardium, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, Transforming growth factor beta, biology.organism_classification, medicine.disease, Disease Models, Animal, Treatment Outcome, Infectious Diseases, Benzamides, Immunology, biology.protein, Medicine, Pyrazoles, medicine.symptom, Research Article

Abstract

Background Chagas disease induced by Trypanosoma cruzi (T. cruzi) infection is a major cause of mortality and morbidity affecting the cardiovascular system for which presently available therapies are largely inadequate. Transforming Growth Factor beta (TGFß) has been involved in several regulatory steps of T. cruzi invasion and in host tissue fibrosis. GW788388 is a new TGFß type I and type II receptor kinase inhibitor that can be orally administered. In the present work, we studied its effects in vivo during the acute phase of experimental Chagas disease. Methodology/Principal Findings Male Swiss mice were infected intraperitoneally with 104 trypomastigotes of T. cruzi (Y strain) and evaluated clinically. We found that this compound given once 3 days post infection (dpi) significantly decreased parasitemia, increased survival, improved cardiac electrical conduction as measured by PR interval in electrocardiography, and restored connexin43 expression. We could further show that cardiac fibrosis development, evaluated by collagen type I and fibronectin expression, could be inhibited by this compound. Interestingly, we further demonstrated that administration of GW788388 at the end of the acute phase (20 dpi) still significantly increased survival and decreased cardiac fibrosis (evaluated by Masson's trichrome staining and collagen type I expression), in a stage when parasite growth is no more central to this event. Conclusion/Significance This work confirms that inhibition of TGFß signaling pathway can be considered as a potential alternative strategy for the treatment of the symptomatic cardiomyopathy found in the acute and chronic phases of Chagas disease., Author Summary Cardiac damage and dysfunction are prominent features in patients with chronic Chagas disease, which is caused by infection with the protozoan parasite Trypanosoma cruzi (T. cruzi) and affects 10–12 million individuals in South and Central America. Our group previously reported that transforming growth factor beta (TGFß) is implicated in several regulatory aspects of T. cruzi invasion and growth and in host tissue fibrosis. In the present work, we evaluated the therapeutic action of an oral inhibitor of TGFß signaling (GW788388) administered during the acute phase of experimental Chagas disease. GW788388 treatment significantly reduced mortality and decreased parasitemia. Electrocardiography showed that GW788388 treatment was effective in protecting the cardiac conduction system, preserving gap junction plaque distribution and avoiding the development of cardiac fibrosis. Inhibition of TGFß signaling in vivo appears to potently decrease T. cruzi infection and to prevent heart damage in a preclinical mouse model. This suggests that this class of molecules may represent a new therapeutic tool for acute and chronic Chagas disease that warrants further pre-clinical exploration. Administration of TGFß inhibitors during chronic infection in mouse models should be further evaluated, and future clinical trials should be envisaged.

Published

2012

4. Combined Treatment of Heterocyclic Analogues and Benznidazole upon Trypanosoma cruzi In Vivo

Author

Ana Carolina Mondaine Rodrigues, David W. Boykin, Chad E. Stephens, Denise da Gama Jaen Batista, Maria de Nazaré Correia Soeiro, Constança Britto, Marcos Meuser Batista, and Gabriel Melo de Oliveira

Subjects

Male, Chagas disease, Trypanosoma, Antifungal Agents, Trypanosoma cruzi, Amidines, lcsh:Medicine, Pathogenesis, Parasitemia, Drug resistance, Protozoology, Pharmacology, Microbiology, Mice, In vivo, parasitic diseases, medicine, Animal mortality, Animals, Chagas Disease, lcsh:Science, Furans, Biology, Microbial Pathogens, Multidisciplinary, biology, Chemistry, lcsh:R, biology.organism_classification, medicine.disease, Trypanocidal Agents, Benzamidines, Drug Combinations, Nitroimidazoles, Benznidazole, Immunology, Toxicity, Parastic Protozoans, lcsh:Q, Parasitology, Research Article, medicine.drug

Abstract

Chagas disease caused by Trypanosoma cruzi is an important cause of mortality and morbidity in Latin America but no vaccines or safe chemotherapeutic agents are available. Combined therapy is envisioned as an ideal approach since it may enhance efficacy by acting upon different cellular targets, may reduce toxicity and minimize the risk of drug resistance. Therefore, we investigated the activity of benznidazole (Bz) in combination with the diamidine prodrug DB289 and in combination with the arylimidamide DB766 upon T. cruzi infection in vivo. The oral treatment of T.cruzi-infected mice with DB289 and Benznidazole (Bz) alone reduced the number of circulating parasites compared with untreated mice by about 70% and 90%, respectively. However, the combination of these two compounds decreased the parasitemia by 99% and protected against animal mortality by 100%, but without providing a parasitological cure. When Bz (p.o) was combined with DB766 (via i.p. route), at least a 99.5% decrease in parasitemia levels was observed. DB766+Bz also provided 100% protection against mice mortality while Bz alone provided about 87% protection. This combined therapy also reduced the tissular lesions induced by T. cruzi infection: Bz alone reduced GPT and CK plasma levels by about 12% and 78% compared to untreated mice group, the combination of Bz with DB766 resulted in a reduction of GPT and CK plasma levels of 56% and 91%. Cure assessment through hemocultive and PCR approaches showed that Bz did not provide a parasitological cure, however, DB766 alone or associated with Bz cured ≥13% of surviving animals.

Published

2011